CN109438315A - A kind of preparation method of capillary - Google Patents

A kind of preparation method of capillary Download PDF

Info

Publication number
CN109438315A
CN109438315A CN201811354213.9A CN201811354213A CN109438315A CN 109438315 A CN109438315 A CN 109438315A CN 201811354213 A CN201811354213 A CN 201811354213A CN 109438315 A CN109438315 A CN 109438315A
Authority
CN
China
Prior art keywords
reaction
capillary
edipa
reaction solution
added
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Pending
Application number
CN201811354213.9A
Other languages
Chinese (zh)
Inventor
严家庆
李丹丹
林楠
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
JIANGSU BAOZONG BAODA PHARMACEUTICAL CO Ltd
Original Assignee
JIANGSU BAOZONG BAODA PHARMACEUTICAL CO Ltd
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by JIANGSU BAOZONG BAODA PHARMACEUTICAL CO Ltd filed Critical JIANGSU BAOZONG BAODA PHARMACEUTICAL CO Ltd
Priority to CN201811354213.9A priority Critical patent/CN109438315A/en
Publication of CN109438315A publication Critical patent/CN109438315A/en
Pending legal-status Critical Current

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D207/00Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom
    • C07D207/02Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom
    • C07D207/30Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having two double bonds between ring members or between ring members and non-ring members
    • C07D207/34Heterocyclic compounds containing five-membered rings not condensed with other rings, with one nitrogen atom as the only ring hetero atom with only hydrogen or carbon atoms directly attached to the ring nitrogen atom having two double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms

Abstract

The invention discloses a kind of preparation methods of capillary.It is characterized by: synthesizing capillary by chlorination, a cyclization reaction, secondary cyclization reaction, bromo-reaction, alkylated reaction using 2- bromopropionitrile, DL- p-chlorophenylglycine as starting material.This method biggest advantage is that easy to operate, easy continuous industrial production, total yield of products are not less than 85%, and purity is higher than 99.5%.

Description

A kind of preparation method of capillary
Technical field
The present invention relates to the preparation fields of capillary and its intermediate, and in particular to a kind of preparation method of capillary.
Background technique
Capillary chemical name is the bromo- 2- rubigan -3- nitrile -1- ethoxymethyl -5- trifluoromethyl pyrpole of 4-, is a kind of New pyrrole insecticides have efficient killing effect to various brill moths, sucking, biting mouth parts pest and acarid.Insect is taking After food or contact, mixed-functional oxidase is changed into insecticidal active compound in insect bodies, target is that insect bodies are thin Mitochondria in born of the same parents makes cell synthesis stop vital functions because lacking energy, eventually leads to pest death.Previous capillary Preparation method, by-product is more, and yield is low.
Summary of the invention
The purpose of the present invention is to provide a kind of preparation methods of capillary.Purity 99.5% can be synthesized using this technique Above capillary bulk pharmaceutical chemicals, in order to achieve the above object, mainly using following technical scheme:
(1) preparation of intermediate 1: the 3- bromopropionitrile that 0.757 times is measured is dissolved in the DMF of 0.789 times of amount, in illumination condition Under be slowly introducing the chlorine of 0.404 times of amount, the 0-15 DEG C of reaction for obtaining intermediate 1 (the bromo- 3- chloroethyl nitrile of 2-) after reaction Liquid, room temperature preservation are spare.
(2) preparation of intermediate 2: 1.0 times of PCPG (DL- p-chlorophenylglycine) being dissolved in the acetonitrile of 3.5 times of amounts, After the phosphorus trichloride of 0.251 times of amount is added dropwise, the trifluoro-acetyl chloride gas slowly that 0.726 times is measured is passed through in reaction system, 15-30 The reaction solution of intermediate 2 (2- trifluoromethyl -4- rubigan -3- oxazoline -5- ketone) DEG C is obtained after reaction, and room temperature is protected It deposits spare.
(3) preparation of intermediate 3: the reaction solution of intermediate 1 is added in 2 reaction solution of intermediate, then to reactant The EDIPA (diisopropylethylamine) of 1.15 times of amounts is added dropwise in system, and 20-30 DEG C obtains (the 2- trifluoromethyl-of intermediate 3 after reaction 4- nitrile -5- rubigan pyrroles) reaction solution, room temperature preservation is spare.
(4) preparation of intermediate 4: the bromine that 0.842 times is measured and the EDIPA (diisopropylethylamine) of 1.023 times of amounts are same When be added drop-wise in the reaction solution of intermediate 3,10-15 DEG C obtains (the bromo- 4- nitrile-of 2- trifluoromethyl -3- of intermediate 4 after reaction 5- rubigan pyrroles) reaction solution, room temperature preservation is spare.
(5) preparation of capillary: the reaction solution solvent acetonitrile of intermediate 4 is evaporated under reduced pressure removing, the first of 3.5 times of amounts is added Benzene, the water washing organic phase of 5.0 times of amounts.The DEM (chloromethane base oxethyl ether) that 0.535 times is measured is added in organic phase, to anti- The EDIPA (diisopropylethylamine) that 0.765 times of amount is added dropwise should be embodied.The 20-30 DEG C of reaction solution for obtaining capillary after reaction.
(6) product crystallizes: the water washing capillary reaction solution measured with 5.0 times, and toluene solvant, distillation knot is then distilled off 7.0 times of methanol are added after beam, are heated to flowing back, Slow cooling crystallization, filtering, filter cake is obtained by drying to arrive capillary product, purity 99.5% or more, total recovery is not less than 85%.
The present invention has the advantages that side reaction is few, total recovery is high, and product purity is 99.5% or more.Intermediate does not need Independent purification process is suitble to scale continuous production.The present invention uses TFAC (trifluoro-acetyl chloride) as acylating reagent, trichlorine Changing phosphorus as dehydrating agent keeps a cyclization reaction conversion ratio and raw material availability all very high.Tradition is replaced with the bromo- 3- chloroethyl nitrile of 2- 2,3-, bis- chloroethyl nitrile as cyclizing agent, make secondary cyclization reaction be more easier to carry out, side reaction is significantly less.In bromo-reaction In, it selects EDIPA (diisopropylethylamine) as catalysts, and catalyst is added dropwise simultaneously with bromine, keeps bromo anti- Should more sufficiently, bromine dosage is greatly decreased.Using boiling point is higher, the better EDIPA (two of hydrophobicity in entire synthesis technology Wopropyl ethyl amine) traditional triethylamine is replaced, make to tie up that sour effect is more preferable, while the recovery utilization rate of organic base greatly improves, work Skill is more environmentally-friendly.It can reach 99.5% or more using the capillary bulk pharmaceutical chemicals purity that this technique synthesizes, be higher than most markets Product purity (97.0%) on sale, is suitble to the production of high-end capillary preparation.The other one big advantage of this synthesis technology is not It needs to carry out independent purification process to intermediate, all intermediates all shift in a solvent, until final filtration goes out solid-like production Product are very suitable to scale industrial production.Make the chemical synthesis route of this technique below:
Specific embodiment
Following typical reaction is used to illustrate the present invention, and technical staff in the art is the present invention simple Replacement or improvement etc. belong within the technical solution that the present invention is protected.
Embodiment 1
(1) preparation of intermediate 1 (the bromo- 3- chloroethyl nitrile of 2-)
The 3- bromopropionitrile of 75.7g is dissolved in the DMF of 78.9g, 40.4g chlorine is slowly introducing under illumination condition, is ventilated Temperature is maintained at 0-15 DEG C in the process.After gas is passed through, 3 hours are kept the temperature at 15 DEG C or so.Centre is obtained after reaction The reaction solution of body 1, room temperature preservation are spare.
(2) preparation of intermediate 2 (2- trifluoromethyl -4- rubigan -3- oxazoline -5- ketone)
The PCPG of 100.0g (DL- p-chlorophenylglycine) is dissolved in 350.0g acetonitrile at room temperature, 25.1g phosphorus trichloride It is added drop-wise in reaction system.72.6g trifluoro-acetyl chloride gas slowly is passed through in reaction system, reaction temperature is controlled in 15-30 ℃.After the completion of gas is passed through, 30 DEG C keep the temperature 2 hours.2 reaction solution of intermediate is obtained after reaction, and room temperature preservation is stand-by.
(3) preparation of intermediate 3 (2- trifluoromethyl -4- nitrile -5- rubigan pyrroles)
The reaction solution of intermediate 1 is added in the reaction solution of intermediate 2, by 115.0g EDIPA (diisopropylethylamine) It is added drop-wise in reaction system, reaction temperature control keeps the temperature 1 hour for 30 DEG C or so after 20-30 DEG C, completion of dropwise addition, after reaction The reaction solution of intermediate 3 is obtained, room temperature preservation is spare.
(4) preparation of intermediate 4 (the bromo- 4- nitrile -5- rubigan pyrroles of 2- trifluoromethyl -3-)
The EDIPA (diisopropylethylamine) of 84.5 bromine and 102.3g are added drop-wise in the reaction solution of intermediate 3 simultaneously, Process control reaction temperature is added dropwise at 10-15 DEG C.After being added dropwise, 15 DEG C or so are stirred 1.5 hours.It obtains after reaction The reaction solution of intermediate 4, room temperature preservation are spare.
(5) preparation of capillary
The reaction solution vacuum distillation of intermediate 4 is removed into acetonitrile solvent, vapo(u)rizing temperature is no more than 55 DEG C.After distillation, 350.0g toluene and 500.0g water is added, stratification after stirring 0.5 hour retains upper organic phase.By the DEM (chlorine of 53.5g Methyl ethoxy ether) it is added in organic phase, 76.5gEDIPA (diisopropylethylamine) is added dropwise to reaction system, process is added dropwise Reaction temperature is controlled at 20-30 DEG C, after being added dropwise, is stirred 2 hours at 30 DEG C or so.It is anti-to obtain capillary after reaction Liquid is answered, room temperature preservation is spare.
(6) crystallization of capillary
500.0g water is added in the reaction solution of capillary, stratification after 0.5 hour is stirred at room temperature, retaining upper layer has Machine phase.The toluene solvant of vacuum distillation removing organic phase, vapo(u)rizing temperature are controlled at 100 DEG C or less.After distillation, it is added 700.0g methanol increases temperature to 65 DEG C or so, all dissolves to solid within stirring 0.5 hour.Temperature is slowly reduced to 10-15 DEG C, temperature-fall period was for about 3 hours.It filters, filter cake is capillary tide product.70 DEG C of hot winds dry 6 hours to obtain capillary to damp product Dry product 189.95g, yield 86.5%, purity 99.7%.
Embodiment 2.
(1) preparation of intermediate 1 (the bromo- 3- chloroethyl nitrile of 2-)
The 3- bromopropionitrile of 151.4g is dissolved in the DMF of 157.8g, 80.8g chlorine is slowly introducing under illumination condition, is led to Temperature is maintained at 0-15 DEG C during gas.After gas is passed through, 3 hours are kept the temperature at 15 DEG C or so.In obtaining after reaction The reaction solution of mesosome 1, room temperature preservation are spare.
(2) preparation of intermediate 2 (2- trifluoromethyl -4- rubigan -3- oxazoline -5- ketone)
The PCPG of 200.0g (DL- p-chlorophenylglycine) 50.2g phosphorus trichloride in 700.0g acetonitrile is dissolved at room temperature to drip It is added in reaction system.145.2g trifluoro-acetyl chloride gas slowly is passed through in reaction system, reaction temperature is controlled in 15-30 ℃.After the completion of gas is passed through, 30 DEG C keep the temperature 2 hours.2 reaction solution of intermediate is obtained after reaction, and room temperature preservation is stand-by.
(3) preparation of intermediate 3
The reaction solution of intermediate 1 is added in the reaction solution of intermediate 2, by 230.0g EDIPA (diisopropylethylamine) It is added drop-wise in reaction system, reaction temperature control keeps the temperature 1 hour for 30 DEG C or so after 20-30 DEG C, completion of dropwise addition, after reaction The reaction solution of intermediate 3 (2- trifluoromethyl -4- nitrile -5- rubigan pyrroles) is obtained, room temperature preservation is spare.
(4) preparation of intermediate 4 (the bromo- 4- nitrile -5- rubigan pyrroles of 2- trifluoromethyl -3-)
The EDIPA (diisopropylethylamine) of 169.0 bromine and 204.6g are added drop-wise to the reaction solution of intermediate 3 simultaneously In, process control reaction temperature is added dropwise at 10-15 DEG C.After being added dropwise, 15 DEG C or so are stirred 1.5 hours.After reaction To the reaction solution of intermediate 4, room temperature preservation is spare.
(5) preparation of capillary
The reaction solution vacuum distillation of intermediate 4 is removed into acetonitrile solvent, vapo(u)rizing temperature is no more than 55 DEG C.After distillation, 700.0g toluene and 1000.0g water is added, stratification after stirring 0.5 hour retains upper organic phase.By the DEM of 107.0g (chloromethane base oxethyl ether) is added in organic phase, and 153.0g EDIPA (diisopropylethylamine) is added dropwise to reaction system, is added dropwise Process control reaction temperature is at 20-30 DEG C, after being added dropwise, stirs 2 hours at 30 DEG C or so.Worm mite is obtained after reaction Nitrile reaction solution, room temperature preservation are spare.
(6) crystallization of capillary
1000.0g water is added in the reaction solution of capillary, stratification after 0.5 hour is stirred at room temperature, retains upper layer Organic phase.The toluene solvant of vacuum distillation removing organic phase, vapo(u)rizing temperature are controlled at 100 DEG C or less.After distillation, it is added 1400.0g methanol increases temperature to 65 DEG C or so, all dissolves to solid within stirring 0.5 hour.Temperature is slowly reduced to 10-15 DEG C, temperature-fall period was for about 3 hours.It filters, filter cake is capillary tide product.70 DEG C of hot winds dry 6 hours to obtain capillary to damp product Dry product 385.2g, yield 87.7%, purity 99.6%.
Embodiment 3.
(1) preparation of intermediate 1 (the bromo- 3- chloroethyl nitrile of 2-)
The 3- bromopropionitrile of 757g is dissolved in the DMF of 789g, 404g chlorine, venting process are slowly introducing under illumination condition Middle temperature is maintained at 0-15 DEG C.After gas is passed through, 3 hours are kept the temperature at 15 DEG C or so.Intermediate 1 is obtained after reaction Reaction solution, room temperature preservation are spare.
(2) preparation of intermediate 2 (2- trifluoromethyl -4- rubigan -3- oxazoline -5- ketone)
The PCPG of 1000g (DL- p-chlorophenylglycine) is dissolved in 3500g acetonitrile at room temperature, 251g phosphorus trichloride is added dropwise Into reaction system.726g trifluoro-acetyl chloride gas slowly is passed through in reaction system, reaction temperature is controlled at 15-30 DEG C.Gas After the completion of body is passed through, 30 DEG C keep the temperature 2 hours.2 reaction solution of intermediate is obtained after reaction, and room temperature preservation is stand-by.
(3) preparation of intermediate 3 (2- trifluoromethyl -4- nitrile -5- rubigan pyrroles)
The reaction solution of intermediate 1 is added in the reaction solution of intermediate 2, by 1150g EDIPA (diisopropylethylamine) It is added drop-wise in reaction system, reaction temperature control keeps the temperature 1 hour for 30 DEG C or so after 20-30 DEG C, completion of dropwise addition, after reaction The reaction solution of intermediate 3 is obtained, room temperature preservation is spare.
(4) preparation of intermediate 4 (the bromo- 4- nitrile -5- rubigan pyrroles of 2- trifluoromethyl -3-)
The EDIPA (diisopropylethylamine) of 845 bromine and 1023g are added drop-wise in the reaction solution of intermediate 3 simultaneously, dripped Add process control reaction temperature at 10-15 DEG C.After being added dropwise, 15 DEG C or so are stirred 1.5 hours.Centre is obtained after reaction The reaction solution of body 4, room temperature preservation are spare.
(5) preparation of capillary
The reaction solution vacuum distillation of intermediate 4 is removed into acetonitrile solvent, vapo(u)rizing temperature is no more than 55 DEG C.After distillation, 3500g toluene and 5000g water is added, stratification after stirring 0.5 hour retains upper organic phase.By the DEM (chloromethane of 535g Base oxethyl ether) it is added in organic phase, 765gEDIPA (diisopropylethylamine) is added dropwise to reaction system, process control is added dropwise Reaction temperature is at 20-30 DEG C, after being added dropwise, stirs 2 hours at 30 DEG C or so.Capillary reaction is obtained after reaction Liquid, room temperature preservation are spare.
(6) crystallization of capillary
5000g water is added in the reaction solution of capillary, stratification after 0.5 hour is stirred at room temperature, retaining upper layer has Machine phase.The toluene solvant of vacuum distillation removing organic phase, vapo(u)rizing temperature are controlled at 100 DEG C or less.After distillation, it is added 7000g methanol increases temperature to 65 DEG C or so, all dissolves to solid within stirring 0.5 hour.Slowly reduce temperature to 10-15 DEG C, Temperature-fall period was for about 3 hours.It filters, filter cake is capillary tide product.70 DEG C of hot winds dry 6 hours to obtain capillary dry product to damp product 1906.8g, yield 87.40%, purity 99.7%.

Claims (7)

1. a kind of synthetic method of capillary, it is characterised in that this method carries out as follows:
2- bromopropionitrile is dissolved in DMF, chlorine is passed through, chlorination occurs under illumination condition, prepares intermediate 1;Intermediate 1 It is the bromo- 3- chloroethyl nitrile of 2-;
PCPG is dissolved in acetonitrile, is first embodied to reaction and phosphorus trichloride is added dropwise, TFAC is then passed through again and a cyclization reaction occurs, Generate intermediate 2;PCPG is DL- p-chlorophenylglycine;TFAC is trifluoro-acetyl chloride;Intermediate 2 is -4- pairs of 2- trifluoromethyl Chlorphenyl -3- oxazoline -5- ketone;
By in the reaction solution of the DMF solution investment intermediate 2 of intermediate 1, it is anti-that the secondary cyclization of EDIPA generation then is added dropwise to system It answers, generates intermediate 3;EDIPA is diisopropylethylamine;Intermediate 3 is 2- trifluoromethyl -4- nitrile -5- rubigan pyrroles;
Bromine is added dropwise simultaneously into 3 reaction solution of intermediate and bromo-reaction occurs for EDIPA.
2. obtaining the reaction solution of intermediate 4 after reaction;Intermediate 4 is the bromo- 4- nitrile -5- rubigan of 2- trifluoromethyl -3- Pyrroles;
By the reaction solution vacuum distillation removing acetonitrile solvent of intermediate 4, toluene and water is then added, stratification after stirring is protected Organic phase is stayed, the toluene solution of intermediate 4 is obtained;DEM is added in the toluene solution of intermediate 4, EDIPA is added dropwise and carries out alkyl Change reaction, generates capillary reaction solution after reaction;DEM is chloromethane base oxethyl ether.
3. a kind of synthetic method of capillary according to claim 1, which is characterized in that in the chlorination with 2- bromopropionitrile is raw material, and intermediate 1 is generated under illumination condition.
4. a kind of synthetic method of capillary according to claim 1, which is characterized in that a cyclization reaction In using TFAC as acylating reagent, phosphorus trichloride is dehydrating agent.
5. a kind of synthetic method of capillary according to claim 1, which is characterized in that the secondary cyclization reaction In with intermediate 1 be cyclizing agent, using EDIPA as acid binding agent.
6. a kind of synthetic method of capillary according to claim 1, which is characterized in that in the bromo-reaction with EDIPA is as catalyst, and catalyst and bromine are added drop-wise in reaction system simultaneously.
7. a kind of synthetic method of capillary according to claim 1, which is characterized in that in the alkylated reaction Using EDIPA as acid binding agent.
CN201811354213.9A 2018-11-14 2018-11-14 A kind of preparation method of capillary Pending CN109438315A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
CN201811354213.9A CN109438315A (en) 2018-11-14 2018-11-14 A kind of preparation method of capillary

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
CN201811354213.9A CN109438315A (en) 2018-11-14 2018-11-14 A kind of preparation method of capillary

Publications (1)

Publication Number Publication Date
CN109438315A true CN109438315A (en) 2019-03-08

Family

ID=65552916

Family Applications (1)

Application Number Title Priority Date Filing Date
CN201811354213.9A Pending CN109438315A (en) 2018-11-14 2018-11-14 A kind of preparation method of capillary

Country Status (1)

Country Link
CN (1) CN109438315A (en)

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN114524758A (en) * 2022-01-12 2022-05-24 山东潍坊双星农药有限公司 Novel synthesis process of chlorfenapyr
CN114573494A (en) * 2022-04-14 2022-06-03 山东潍坊双星农药有限公司 Preparation method of chlorfenapyr
WO2023197562A1 (en) * 2022-04-15 2023-10-19 陕西美邦药业集团股份有限公司 Preparation method for chlorfenapyr and analog thereof

Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2682504A (en) * 1952-01-02 1954-06-29 Minnesota Mining & Mfg Preparation of monochloropropionic acid
CN101591284A (en) * 2009-06-29 2009-12-02 湖南化工研究院 The preparation method of bromothalonil and analogue thereof
CN102617439A (en) * 2012-02-27 2012-08-01 山东潍坊双星农药有限公司 Preparation method of chlorfenapyr
WO2018166819A1 (en) * 2017-03-13 2018-09-20 BASF Agro B.V. Production of arylpyrrol compounds in the presence of dipea base

Patent Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2682504A (en) * 1952-01-02 1954-06-29 Minnesota Mining & Mfg Preparation of monochloropropionic acid
CN101591284A (en) * 2009-06-29 2009-12-02 湖南化工研究院 The preparation method of bromothalonil and analogue thereof
CN102617439A (en) * 2012-02-27 2012-08-01 山东潍坊双星农药有限公司 Preparation method of chlorfenapyr
WO2018166819A1 (en) * 2017-03-13 2018-09-20 BASF Agro B.V. Production of arylpyrrol compounds in the presence of dipea base

Non-Patent Citations (3)

* Cited by examiner, † Cited by third party
Title
JUSTIN Y. SU ET AL.: "Synthetic Studies Toward Pactamycin Highlighting Oxidative C−H and Alkene Amination Technologies", 《THE JOURNAL OF ORGANIC CHEMISTRY》 *
付庆等: "溴虫腈的合成", 《农药》 *
高鸿宾等: "《有机活性中间体》", 30 November 1987, 高等教育出版社 *

Cited By (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN114524758A (en) * 2022-01-12 2022-05-24 山东潍坊双星农药有限公司 Novel synthesis process of chlorfenapyr
CN114573494A (en) * 2022-04-14 2022-06-03 山东潍坊双星农药有限公司 Preparation method of chlorfenapyr
CN114573494B (en) * 2022-04-14 2024-03-15 山东潍坊双星农药有限公司 Preparation method of chlorfenapyr
WO2023197562A1 (en) * 2022-04-15 2023-10-19 陕西美邦药业集团股份有限公司 Preparation method for chlorfenapyr and analog thereof

Similar Documents

Publication Publication Date Title
CN109438315A (en) A kind of preparation method of capillary
CN102827042B (en) Chiral synthesis method of florfenicol
CN108546258B (en) A kind of method that simple and effective synthesizes esterdiol in Corey
CN107857741A (en) The new technique for synthesizing of ainothiazoly loximate
CN107963993A (en) A kind of preparation method of high-purity ethiprole
CN101481332B (en) Method for synthesizing alkoxy aromatic amidine compounds
CN112062712A (en) Preparation method of 2- (5-bromo-3-methylpyridin-2-yl) acetic acid hydrochloride
CN103613535A (en) Synthesis method of 5-(methoxy methyl)-2,3-pyridine dimethyl dicarboxylate
CN109897064B (en) Preparation method of 3-indolyl-3- (phosphodiethyl) oxoindole compound
CN113181850A (en) Microchannel preparation method of indole compound
CN108033903A (en) Synthesis process for D L-p-methylsulfonylphenylserine ethyl ester with water esterification
CN101550097B (en) Preparation method of 5-chlorosulfonyl isophthaloyl acid chloride
CN109053491A (en) Synthetic method of the acaricide cyflumetofen intermediate to tert-butyl benzene acetonitrile
CN112645894B (en) Method for preparing sulpirazole intermediate 5, 5-dimethyl-4, 5-dihydroisoxazole-3-thiocarboxamidine hydrochloride
CN105085469B (en) A kind of preparation method of the carboxylic acid of 5 chlorothiophene 2
CN109748826B (en) Synthetic method of indoxacarb intermediate hydrazinobenzyl formate
CN108976214A (en) Pyruvate dehydrogenase system inhibitor and its preparation method and application
CN106905161B (en) A kind of synthetic method of 2- chlorine-4-fluorine-5-nitro benzoic acid
CN106518865A (en) Method for preparing 1-alkenyl indolizine derivative
CN101020645A (en) Prepn process of diethylamino ethanol caproate
CN112645863A (en) Dipyrromethene-1-one compounds and preparation method thereof
CN113372228B (en) Preparation method of 2-amino-6-chloro-4-nitrophenol
CN105017252A (en) 1,3,8-triazaspiro[4,5]decane-2-guanidine-4-ketone compound with biological activity, preparation method therefor and application thereof
CN109942584B (en) Method for synthesizing Becrabavir intermediate
CN104418760A (en) Method for continuous water removal production of amide product

Legal Events

Date Code Title Description
PB01 Publication
PB01 Publication
SE01 Entry into force of request for substantive examination
SE01 Entry into force of request for substantive examination
RJ01 Rejection of invention patent application after publication
RJ01 Rejection of invention patent application after publication

Application publication date: 20190308